Cytomegalovirus-infected human endothelial cells can stimulate allogeneic CD4+ memory T cells by releasing antigenic exosomes

JD Walker, CL Maier, JS Pober - The Journal of Immunology, 2009 - journals.aai.org
JD Walker, CL Maier, JS Pober
The Journal of Immunology, 2009journals.aai.org
Human CMV infection is controlled by T cell-mediated immunity and in immunosuppressed
transplant patients it is associated with acute allograft rejection as well as chronic allograft
vasculopathy. CMV infects endothelial cells (EC) and it is thought that CMV-specific host
immune responses to infected allograft EC contribute to rejection. In vitro, CD4+ T cells from
CMV-positive donors (but not CMV-negative donors) are readily activated by CMV-infected
allogeneic EC, although it is unclear how allogeneic CMV-infected EC activate self-class II …
Abstract
Human CMV infection is controlled by T cell-mediated immunity and in immunosuppressed transplant patients it is associated with acute allograft rejection as well as chronic allograft vasculopathy. CMV infects endothelial cells (EC) and it is thought that CMV-specific host immune responses to infected allograft EC contribute to rejection. In vitro, CD4+ T cells from CMV-positive donors (but not CMV-negative donors) are readily activated by CMV-infected allogeneic EC, although it is unclear how allogeneic CMV-infected EC activate self-class II MHC-restricted memory CD4+ T cells. In this study, we confirm that purified CD4+ T cells from CMV+ donors are activated by allogeneic CMV-infected EC, but find that the response is dependent upon copurified APC expressing class II MHC that are autologous to the T cells. The transfer of CMV Ags from infected EC to APC can be mediated by EC-derived exosome-like particles. These results provide a mechanism by which CMV can exacerbate allograft rejection and suggest a novel function of EC-derived exosomes that could contribute in a more general manner to immune surveillance.
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